Haworth R A, Goknur A B
Department of Anesthesiology, University of Wisconsin Medical School, Madison, USA.
Anesthesiology. 1995 May;82(5):1255-65. doi: 10.1097/00000542-199505000-00021.
Volatile anesthetics exert profound effects on the heart, probably through their effect on Ca2+ movements during the cardiac cycle. Ca2+ movements across the sarcolemma are thought to involve mainly Ca2+ channels and the Na+/Ca2+ exchanger. We have therefore investigated the action of halothane, isoflurane, and enflurane on Na+/Ca2+ exchange and Ca2+ channel activity to assess the contribution of these pathways to the observed effect of the anesthetics on the myocardium.
Sarcolemmal ion fluxes were investigated using radioisotope uptake by isolated adult rat heart cells in suspension. Na+/Ca2+ exchange activity was measured from 45Ca2+ uptake by Na(+)-loaded cells. Ca2+ channel activity was measured from verapamil-sensitive trace 54Mn2+ uptake during electric stimulation.
Halothane, isoflurane, and enflurane inhibited Na+/Ca2+ exchange completely, with similar potency when concentrations were expressed in millimolar units in aqueous medium but not when expressed as minimum alveolar concentration (MAC). The inhibition by enflurane was particularly strong, > 50%, at 2 MAC. In contrast, the three anesthetics inhibited Ca2+ channels with similar potency when concentrations were expressed as MAC but not when expressed in millimolar units in aqueous medium. Hill plots of pooled data with all three anesthetics showed a slope of -3.87 +/- 0.50 for inhibition of Na+/Ca2+ exchange and -1.73 +/- 0.19 for inhibition of Ca2+ channels.
Halothane, isoflurane, and enflurane inhibit both Na+/Ca2+ exchange and Ca2+ channels at concentrations relevant to anesthesia, although they exhibit differences in potency and number of sites of action. At 1.5 MAC, halothane inhibits Ca2+ channels more than Na+/Ca2+ exchange, whereas enflurane inhibits Na+/Ca2+ exchange more than Ca2+ channels. Isoflurane inhibited both systems equally. The inhibition of Ca2+ influx by these agents is likely to contribute to their negative inotropic effect in the heart. The inhibition of Na+/Ca2+ exchange by enflurane may account for its observed action of delaying relaxation in species lacking sarcoplasmic reticulum.
挥发性麻醉药对心脏有深远影响,可能是通过其在心动周期中对Ca2+运动的作用。跨肌膜的Ca2+运动主要被认为涉及Ca2+通道和Na+/Ca2+交换体。因此,我们研究了氟烷、异氟烷和恩氟烷对Na+/Ca2+交换和Ca2+通道活性的作用,以评估这些途径对观察到的麻醉药对心肌作用的贡献。
使用悬浮的成年大鼠心脏分离细胞的放射性同位素摄取来研究肌膜离子通量。通过Na+负载细胞摄取45Ca2+来测量Na+/Ca2+交换活性。在电刺激期间,通过维拉帕米敏感的微量54Mn2+摄取来测量Ca2+通道活性。
氟烷、异氟烷和恩氟烷完全抑制Na+/Ca2+交换,当浓度以水介质中的毫摩尔单位表示时,它们的效力相似,但以最低肺泡浓度(MAC)表示时则不然。恩氟烷在2 MAC时的抑制作用特别强,>50%。相比之下,当浓度以MAC表示时,这三种麻醉药抑制Ca2+通道的效力相似,但以水介质中的毫摩尔单位表示时则不然。将所有三种麻醉药的汇总数据绘制的希尔图显示,抑制Na+/Ca2+交换的斜率为-3.87±0.50,抑制Ca2+通道的斜率为-1.73±0.19。
氟烷、异氟烷和恩氟烷在与麻醉相关的浓度下均抑制Na+/Ca2+交换和Ca2+通道,尽管它们在效力和作用位点数量上存在差异。在1.5 MAC时,氟烷对Ca2+通道的抑制作用大于对Na+/Ca2+交换的抑制作用,而恩氟烷对Na+/Ca2+交换的抑制作用大于对Ca2+通道的抑制作用。异氟烷对这两个系统的抑制作用相同。这些药物对Ca2+内流的抑制可能导致它们对心脏的负性肌力作用。恩氟烷对Na+/Ca2+交换的抑制可能解释了其在缺乏肌浆网的物种中观察到的延迟舒张作用。
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